Your search keyword '"Ralf, Kist"' showing total 31 results

1. Msx1 haploinsufficiency modifies the Pax9-deficient cardiovascular phenotype

Author

Ramada R. Khasawneh, Simon D. Bamforth, Helen M. Phillips, Timothy J. Mohun, Jürgen E. Schneider, Stéphane Zaffran, Heiko Peters, Ralf Kist, Rachel Queen, Rafiqul Hussain, Jonathan Coxhead, Newcastle University [Newcastle], Yarmouk University (YU), University of Leeds, The Francis Crick Institute [London], Marseille medical genetics - Centre de génétique médicale de Marseille (MMG), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), and Malbec, Odile

Subjects

Model organisms, Aortic arch, Pathology, medicine.medical_specialty, QH301-705.5, [SDV]Life Sciences [q-bio], Cardiovascular development, Pharyngeal endoderm, Haploinsufficiency, Biology, Cardiovascular System, Imaging, 03 medical and health sciences, Mice, Neural crest, 0302 clinical medicine, medicine.artery, medicine, Animals, Biology (General), 030304 developmental biology, MSX1 Transcription Factor, Mice, Knockout, 0303 health sciences, Research, Hyoid bone, Embryogenesis, Interrupted aortic arch, medicine.disease, Pax9, [SDV] Life Sciences [q-bio], stomatognathic diseases, medicine.anatomical_structure, Branchial Region, Phenotype, PAX9 Transcription Factor, Neural crest cell migration, 030217 neurology & neurosurgery, Msx1, Developmental Biology, Artery

Abstract

Background Successful embryogenesis relies on the coordinated interaction between genes and tissues. The transcription factors Pax9 and Msx1 genetically interact during mouse craniofacial morphogenesis, and mice deficient for either gene display abnormal tooth and palate development. Pax9 is expressed specifically in the pharyngeal endoderm at mid-embryogenesis, and mice deficient for Pax9 on a C57Bl/6 genetic background also have cardiovascular defects affecting the outflow tract and aortic arch arteries giving double-outlet right ventricle, absent common carotid arteries and interruption of the aortic arch. Results In this study we have investigated both the effect of a different genetic background and Msx1 haploinsufficiency on the presentation of the Pax9-deficient cardiovascular phenotype. Compared to mice on a C57Bl/6 background, congenic CD1-Pax9–/– mice displayed a significantly reduced incidence of outflow tract defects but aortic arch defects were unchanged. Pax9–/– mice with Msx1 haploinsufficiency, however, have a reduced incidence of interrupted aortic arch, but more cases with cervical origins of the right subclavian artery and aortic arch, than seen in Pax9–/– mice. This alteration in arch artery defects was accompanied by a rescue in third pharyngeal arch neural crest cell migration and smooth muscle cell coverage of the third pharyngeal arch arteries. Although this change in phenotype could theoretically be compatible with post-natal survival, using tissue-specific inactivation of Pax9 to maintain correct palate development whilst inducing the cardiovascular defects was unable to prevent postnatal death in the mutant mice. Hyoid bone and thyroid cartilage formation were abnormal in Pax9–/– mice. Conclusions Msx1 haploinsufficiency mitigates the arch artery defects in Pax9–/– mice, potentially by maintaining the survival of the 3rd arch artery through unimpaired migration of neural crest cells to the third pharyngeal arches. With the neural crest cell derived hyoid bone and thyroid cartilage also being defective in Pax9–/– mice, we speculate that the pharyngeal endoderm is a key signalling centre that impacts on neural crest cell behaviour highlighting the ability of cells in different tissues to act synergistically or antagonistically during embryo development.

Published

2021

2. Gene expression changes associated with malignant transformation of oral potentially malignant disorders

Author

John Casement, Hans Prakash Sathasivam, Ralf Kist, Peter Thomson, Timothy C. Bates, Max Robinson, and Philip Sloan

Subjects

Cancer Research, Candidate gene, Biopsy, Cell, Gene Expression, Biology, Pathology and Forensic Medicine, Malignant transformation, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Gene expression, medicine, Humans, Gene, RNA, 030206 dentistry, Fold change, Cell Transformation, Neoplastic, medicine.anatomical_structure, Otorhinolaryngology, 030220 oncology & carcinogenesis, Carcinoma, Squamous Cell, Cancer research, Periodontics, Mouth Neoplasms, Oral Surgery

Abstract

Background: A large number of oral squamous cell carcinomas (OSCCs) are believed to be preceded by oral potentially malignant disorders (OPMD) that have an increased likelihood of malignant transformation compared to clinically normal mucosa. This study was performed to identify differentially expressed genes between OPMDs that underwent malignant transformation (MT) and those that did not, termed “non-transforming” (NT) cases. Methods: Total RNA was extracted from formalin-fixed paraffin-embedded tissue biopsies of 20 OPMD cases with known clinical outcomes (10 MT vs. 10 NT). Samples were assessed for quantity, quality and integrity of RNA prior to sequencing. Analysis for differential gene expression between MT and NT was performed using statistical packages in R. Genes were considered to be significantly differentially expressed if the False Discovery Rate corrected P-value was 1.90). Analysis of RNA-Sequencing outputs revealed 41 genes (34 protein-coding; 7 non-coding) that were significantly differentially expressed between MT and NT cases. The log2 fold change for the statistically significant differentially expressed genes ranged from −2.63 to 2.48, with 23 protein-coding genes being downregulated and 11 protein-coding genes being upregulated in MT cases compared to NT cases. Conclusion: Several candidate genes that may play a role in malignant transformation of OPMD have been identified. Experiments to validate these candidates are underway. It is anticipated that this work will contribute to better understanding of the etiopathogenesis of OPMD and development of novel biomarkers.

Published

2020

3. Metalloprotease-Dependent Attenuation of BMP Signaling Restricts Cardiac Neural Crest Cell Fate

Author

Takuya Yamamoto, Fuminori Sato, Atsuko Sehara-Fujisawa, Haruhiko Akiyama, Hiroshi Kiyonari, Yuki Yoshimoto, Hiroyuki Arai, Ralf Kist, Knut Woltjen, and Chisa Shukunami

Subjects

0301 basic medicine, animal structures, Bone Morphogenetic Protein 6, cardiac neural crest cells, SOX9, a disintegrin and metalloprotease 19, Alk2, ACVR1, Bone morphogenetic protein, General Biochemistry, Genetics and Molecular Biology, Proto-Oncogene Proteins c-myc, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, medicine, Animals, Humans, lcsh:QH301-705.5, Mice, Knockout, Metalloproteinase, Chemistry, Cardiac neural crest cells, Myocardium, Neural crest, bone morphogenic protein, Cell Differentiation, SOX9 Transcription Factor, Embryo, Mammalian, Chondrogenesis, Up-Regulation, Cell biology, skeletogenesis, ADAM Proteins, Cartilage, HEK293 Cells, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), Neural Crest, embryonic structures, Activin Receptors, Type I, 030217 neurology & neurosurgery, Signal Transduction, Sox9

Abstract

In higher vertebrates, cephalic neural crest cells (NCCs) form craniofacial skeleton by differentiating into chondrocytes and osteoblasts. A subpopulation of cephalic NCCs, cardiac NCCs (CNCCs), migrates to the heart. However, CNCCs mostly do not yield skeletogenic derivatives, and the molecular mechanisms of this fate restriction remain elusive. We identify a disintegrin and metalloprotease 19 (Adam19) as a position-specific fate regulator of NCCs. Adam19-depleted mice abnormally form NCC-derived cartilage in their hearts through the upregulation of Sox9 levels in CNCCs. Moreover, NCC-lineage-specific Sox9-overexpressing mice recapitulate CNCC chondrogenesis. In vitro experiments show that Adam19 mediates the cleavage of bone morphogenic protein (BMP) type I receptor Alk2 (Acvr1), whereas pharmacogenetic approaches reveal that Adam19 inhibits CNCC chondrogenesis by suppressing the BMP-Sox9 cascade, presumably through processing Alk2. These findings suggest a metalloprotease-dependent mechanism attenuating cellular responsiveness to BMP ligands, which is essential for both the positional restriction of NCC skeletogenesis and normal heart development., 心臓内での軟骨形成をおさえる仕組みを解明 --プロテアーゼが細胞の軟骨分化を防ぐ--. 京都大学プレスリリース. 2019-10-21.

Published

2019

4. Predicting the clinical outcome of oral potentially malignant disorders using transcriptomic-based molecular pathology

Author

Peter Thomson, John Alexander, Ralf Kist, Michael Nugent, Syed Haider, Max Robinson, Hans Prakash Sathasivam, and Philip Sloan

Subjects

Oncology, Male, Cancer Research, medicine.medical_specialty, Epithelial dysplasia, Tissue Fixation, Biopsy, Proof of Concept Study, Article, Malignant transformation, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Gene Regulatory Networks, Aged, Training set, Paraffin Embedding, Data normalisation, Molecular pathology, business.industry, Sequence Analysis, RNA, Gene Expression Profiling, Gene signature, Middle Aged, Prognosis, Survival Analysis, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, 030220 oncology & carcinogenesis, Test set, Female, Mouth Neoplasms, business

Abstract

BACKGROUND: This study was undertaken to develop and validate a gene expression signature that characterises oral potentially malignant disorders (OPMD) with a high risk of undergoing malignant transformation. METHODS: Patients with oral epithelial dysplasia at one hospital were selected as the ‘training set’ (n = 56) whilst those at another hospital were selected for the ‘test set’ (n = 66). RNA was extracted from formalin-fixed paraffin-embedded (FFPE) diagnostic biopsies and analysed using the NanoString nCounter platform. A targeted panel of 42 genes selected on their association with oral carcinogenesis was used to develop a prognostic gene signature. Following data normalisation, uni- and multivariable analysis, as well as prognostic modelling, were employed to develop and validate the gene signature. RESULTS: A prognostic classifier composed of 11 genes was developed using the training set. The multivariable prognostic model was used to predict patient risk scores in the test set. The prognostic gene signature was an independent predictor of malignant transformation when assessed in the test set, with the high-risk group showing worse prognosis [Hazard ratio = 12.65, p = 0.0003]. CONCLUSIONS: This study demonstrates proof of principle that RNA extracted from FFPE diagnostic biopsies of OPMD, when analysed on the NanoString nCounter platform, can be used to generate a molecular classifier that stratifies the risk of malignant transformation with promising clinical utility.

Published

2020

5. Msx1 deficiency interacts with hypoxia and induces a morphogenetic regulation during lip development

Author

Ralf Kist, Kerstin U. Ludwig, Heiko Peters, Hayato Ohshima, Elisabeth Mangold, Mitsushiro Nakatomi, Steven Lisgo, and Michael Knapp

Subjects

0303 health sciences, Gwas data, 030305 genetics & heredity, Morphogenesis, Embryo, Hypoxia (medical), Biology, Embryonic stem cell, Cell biology, stomatognathic diseases, 03 medical and health sciences, medicine, medicine.symptom, Molecular Biology, PAX9, Gene, Psychological repression, 030304 developmental biology, Developmental Biology

Abstract

Nonsyndromic clefts of the lip and palate are common birth defects resulting from gene-gene and gene-environment interactions. Mutations in human MSX1 have been linked to orofacial clefting and we show here that Msx1 deficiency causes a growth defect of the medial nasal process (Mnp) in mouse embryos. Although this defect alone does not disrupt lip formation, Msx1-deficient embryos develop a cleft lip when the mother is transiently exposed to reduced oxygen levels or to phenytoin, a drug known to cause embryonic hypoxia. In the absence of interacting environmental factors, the Mnp growth defect caused by Msx1 deficiency is modified by a Pax9-dependent 'morphogenetic regulation', which modulates Mnp shape, rescues lip formation and involves a localized abrogation of Bmp4-mediated repression of Pax9 Analyses of GWAS data revealed a genome-wide significant association of a Gene Ontology morphogenesis term (including assigned roles for MSX1, MSX2, PAX9, BMP4 and GREM1) specifically for nonsyndromic cleft lip with cleft palate. Our data indicate that MSX1 mutations could increase the risk for cleft lip formation by interacting with an impaired morphogenetic regulation that adjusts Mnp shape, or through interactions that inhibit Mnp growth.

Published

2020

6. PAX9 regulates squamous cell differentiation and carcinogenesis in the oro-oesophageal epithelium

Author

Xiaoxin Chen, Zhaohui Xiong, Joab Otieno Odera, Zheng Sun, Heiko Peters, Hao Chen, Yawan Lyvia Zhang, Tong Chen, Caizhi Huang, Ralf Kist, Katherine S. Garman, Shuang Ren, and Yao Liu

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Cell growth, Cellular differentiation, Cell, Biology, medicine.disease_cause, Epithelium, Pathology and Forensic Medicine, stomatognathic diseases, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Downregulation and upregulation, Cancer research, medicine, Carcinogenesis, Transcription factor, PAX9

Abstract

PAX9 is a transcription factor of the PAX family characterized by a DNA-binding paired domain. Previous studies have suggested a potential role of PAX9 in squamous cell differentiation and carcinogenesis of the oro-oesophageal epithelium. However, its functional roles in differentiation and carcinogenesis remain unclear. In this study, Pax9 deficiency in mouse oesophagus promoted cell proliferation, delayed cell differentiation, and altered the global gene expression profile. Ethanol exposure downregulated PAX9 expression in human oesophageal epithelial cells in vitro and mouse forestomach and tongue in vivo. We further showed that PAX9 was downregulated in human oro-oesophageal squamous cell carcinoma (OESCC), and its downregulation was associated with alcohol drinking and promoter hypermethylation. Moreover, ad libitum feeding with a liquid diet containing ethanol for 40 weeks or Pax9 deficiency promoted N-nitrosomethylbenzylamine-induced squamous cell carcinogenesis in mouse tongue, oesophagus, and forestomach. In conclusion, PAX9 regulates squamous cell differentiation in the oro-oesophageal epithelium. Alcohol drinking and promoter hypermethylation are associated with PAX9 silencing in human OESCC. PAX9 downregulation may contribute to alcohol-associated oro-oesophageal squamous cell carcinogenesis. Copyright © 2017 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published

2017

7. Pax9 is required for cardiovascular development and interacts with Tbx1 in the pharyngeal endoderm to control 4th pharyngeal arch artery morphogenesis

Author

Anastasia I. Kousa, Catherine A. Stothard, Ralf Kist, Helen M. Phillips, J. Alberto Briones-Leon, Kerstin Seidel, Timothy Bates, Timothy J. Mohun, René Maehr, Mitsushiro Nakatomi, Rebecca Dodds, Simon Cockell, Rachel Sanders, Heiko Peters, Wasay Mohiuddin Shaikh Qureshi, Ramada R. Khasawneh, Simon D. Bamforth, Jürgen E. Schneider, and Silvia Mazzotta

Subjects

TBX1, Aortic arch, Interrupted aortic arch, Anatomy, Biology, medicine.disease, Pharyngeal arch artery morphogenesis, stomatognathic diseases, medicine.anatomical_structure, stomatognathic system, DiGeorge syndrome, medicine.artery, embryonic structures, medicine, Endoderm, Pharyngeal arch, Artery

Abstract

Developmental defects affecting the heart and aortic arch arteries are a key phenotype observed in DiGeorge syndrome patients and are caused by a microdeletion on chromosome 22q11. Heterozygosity ofTBX1, one of the deleted genes, is expressed throughout the pharyngeal arches and is considered a key component for the arch artery defects.Pax9is expressed in the pharyngeal endoderm and is downregulated inTbx1mutant mice. We show here thatPax9deficient mice are born with complex cardiovascular malformations affecting the outflow tract and aortic arch arteries with failure of the 3rdand 4thpharyngeal arch arteries to form correctly. Transcriptome analysis indicated thatPax9andTbx1may function together, and mice double heterozygous forTbx1/Pax9presented with a significantly increased incidence of interrupted aortic arch when compared toTbx1heterozygous mice. Using a novelPax9Creallele we demonstrated that the site of thisTbx1-Pax9genetic interaction is in the pharyngeal endoderm, therefore revealing that aTbx1/Pax9-controlled signalling mechanism emanating from the pharyngeal endoderm is required for critical tissue interactions during normal morphogenesis of the pharyngeal arch artery system.Summary statementPax9is required for outflow tract and aortic arch development, and functions together withTbx1in the pharyngeal endoderm for 4tharch artery formation.

Published

2019

8. Electronic Cigarettes and Oral Health

Author

Benjamin W. Chaffee, P M Preshaw, Richard Holliday, Nicholas S. Jakubovics, and Ralf Kist

Subjects

medicine.medical_specialty, medicine.medical_treatment, Reviews, Electronic Nicotine Delivery Systems, Oral health, tobacco, Tobacco smoke, Nicotine, 03 medical and health sciences, 0302 clinical medicine, Environmental health, Epidemiology, medicine, dental research, Clinical significance, 030212 general & internal medicine, Microbiome, General Dentistry, business.industry, Smoking, 030206 dentistry, Critical Reviews in Oral Biology & Medicine, Clinical trial, Cross-Sectional Studies, oral health, Smoking cessation, Smoking Cessation, business, periodontal diseases, nicotine, medicine.drug

Abstract

Novel nicotine products, particularly electronic cigarettes (e-cigarettes), have become increasingly popular over the past decade. E-cigarettes are sometimes regarded as a less harmful alternative to tobacco smoking, and there is some evidence of their potential role as a smoking cessation aid. However, there are concerns about their health consequences, particularly in users who are not tobacco smokers, and also when used long term. Given the mode of delivery of these products, there is potential for oral health consequences. Over the past few years, there have been an increasing number of studies conducted to explore their oral health effects. In vitro studies have reported a range of cellular effects, but these are much less pronounced than those resulting from exposure to tobacco smoke. Microbiological studies have indicated that e-cigarette users have a distinct microbiome, and there is some indication this may be more pathogenic compared to nonusers. Evidence of oral health effects from clinical trials is still limited, and most studies to date have been small in scale and usually cross-sectional in design. Epidemiological studies highlight concerns over oral dryness, irritation, and gingival diseases. Interpreting data from e-cigarette studies is challenging, given the different populations that have been investigated and the continual emergence of new products. Overall, studies reveal potential oral health harms, underscoring the importance of efforts to reduce use in nonsmokers. However, in smokers who are using e-cigarettes as an aid to help them quit, the benefits of quitting tobacco smoking may outweigh any negative oral health impacts of e-cigarette use, particularly in the short term. Future research is needed to understand the clinical significance of some of the biological changes observed by following different cohorts of users longitudinally in carefully designed clinical studies and pragmatic trials supported by high-quality in vitro studies.

Published

2021

9. Generation of Pax1/PAX1-Specific Monoclonal Antibodies

Author

Amy Middleton, Elisabeth Kremmer, Regina Feederle, Josef-Karl Gerber, Ralf Kist, Heiko Peters, and Emily Northrup

Subjects

0301 basic medicine, Cell type, medicine.diagnostic_test, medicine.drug_class, Immunology, Pax genes, Methylation, Biology, Monoclonal antibody, Molecular biology, 03 medical and health sciences, 030104 developmental biology, Western blot, medicine, Immunology and Allergy, Immunohistochemistry, Transcription factor, PAX9

Abstract

Pax genes encode an evolutionary conserved group of transcription factors with multiple roles during embryonic development and for cell type specification in normal and malignant tissues of the adult organism. In mice, Pax1 is required for the formation of specific skeletal structures as well as for the development of a fully functional thymus. In humans, the PAX1 locus has been linked to otofaciocervical syndrome, idiopathic scoliosis, and to a higher susceptibility for androgenic alopecia. In addition, the methylation status of PAX1 has recently emerged as a sensitive marker for predictive screening of cervical cancer. To provide a reagent for reproducible detection of Pax1 expression, we have generated rat monoclonal antibodies (MAbs) against the murine Pax1 protein. MAbs of one clone (clone 5A2) specifically detect mouse Pax1 protein in Western blot analyses. Moreover, the anti-Pax1 MAbs cross-react with human PAX1 protein and are applicable in immunohistochemical detection procedures using paraformaldehyde/formalin-fixed tissues embedded in paraffin. The anti-Pax1 MAbs provide a reliable reagent for reproducible Pax1/PAX1 protein expression analyses and, therefore, may help to improve diagnostic protocols in clinical settings involving deregulated expression of Pax1/PAX1.

Published

2016

10. Changes in Epidermal Growth Factor Receptor Gene Copy Number during Oral Carcinogenesis

Author

Philip Sloan, Max Robinson, Timothy Bates, Selvam Thavaraj, Matthew Kennedy, Emma Doran, Ralf Kist, Michaela Goodson, Peter Thomson, Ameena Ryhan Diajil, and Heather Farrimond

Subjects

Adult, Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Carcinogenesis, Epidemiology, Gene Dosage, Bioinformatics, medicine.disease_cause, Gene dosage, Malignant transformation, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Epidermal growth factor receptor, Copy-number variation, Aged, Aged, 80 and over, Mouth neoplasm, biology, business.industry, Cancer, Middle Aged, medicine.disease, ErbB Receptors, 030104 developmental biology, ROC Curve, 030220 oncology & carcinogenesis, Carcinoma, Squamous Cell, biology.protein, Biomarker (medicine), Female, Mouth Neoplasms, business, Biomarkers

Abstract

Background: Oral squamous cell carcinoma (OSCC) is a global healthcare problem associated with poor clinical outcomes. Early detection is key to improving patient survival. OSCC may be preceded by clinically recognizable lesions, termed oral potentially malignant disorders (OPMD). As histologic assessment of OPMD does not accurately predict their clinical behavior, biomarkers are required to detect cases at risk of malignant transformation. Epidermal growth factor receptor gene copy number (EGFR GCN) is a validated biomarker in lung non–small cell carcinoma. We examined EGFR GCN in OPMD and OSCC to determine its potential as a biomarker in oral carcinogenesis. Methods: EGFR GCN was examined by in situ hybridization (ISH) in biopsies from 78 patients with OPMD and 92 patients with early-stage (stages I and II) OSCC. EGFR ISH signals were scored by two pathologists and a category assigned by consensus. The data were correlated with patient demographics and clinical outcomes. Results: OPMD with abnormal EGFR GCN were more likely to undergo malignant transformation than diploid cases. EGFR genomic gain was detected in a quarter of early-stage OSCC, but did not correlate with clinical outcomes. Conclusion: These data suggest that abnormal EGFR GCN has clinical utility as a biomarker for the detection of OPMD destined to undergo malignant transformation. Prospective studies are required to verify this finding. It remains to be determined if EGFR GCN could be used to select patients for EGFR-targeted therapies. Impact: Abnormal EGFR GCN is a potential biomarker for identifying OPMD that are at risk of malignant transformation. Cancer Epidemiol Biomarkers Prev; 25(6); 927–35. ©2016 AACR.

Published

2016

11. PROGNOSTIC CLASSIfiER FOR ORAL POTENTIALLY MALIGNANT DISORDERS: AN INTEGRATED HISTOPATHOLOGICAL AND MOLECULAR APPROACH

Author

Ralf Kist, Philip Sloan, Hans Prakash Sathasivam, and Max Robinson

Subjects

Oncology, False discovery rate, medicine.medical_specialty, Epithelial dysplasia, Normal oral mucosa, business.industry, Pathology and Forensic Medicine, Malignant transformation, Loss of heterozygosity, Molecular classification, Internal medicine, Cohort, Medicine, Radiology, Nuclear Medicine and imaging, Dentistry (miscellaneous), Surgery, In patient, Oral Surgery, business

Abstract

Objectives Oral squamous cell carcinoma (OSCC) is associated with a high degree of morbidity and mortality. OS-CCs are often preceded by oral potentially malignant disorders (OPMD) which have a higher propensity to undergo malignant transformation (MT) compared to clinically normal oral mucosa. Currently there is no reliable method to determine which OPMD cases will undergo MT. This study was performed to construct a prognostic classifier for patients with OPMD by integrating clinical, histopathological and molecular factors and to discover a gene expression signature that characterises OPMD with a high risk of undergoing MT. Findings Statistical analysis of an OPMD patient cohort (23 MT vs. 25 with no MT) showed that site of initial OPMD (p = 0.043), binary oral epithelial dysplasia (OED) grading (p = 0.009) and loss of heterozygosity at 3p/9p/17p (p = 0.026) were statistically significant. Other demographic factors, clinical features and the WHO 3-tiered OED grading system were not statistically significant. Gene expression experiments revealed several genes that were differentially expressed between OPMD that underwent MT and those that did not [false discovery rate of Conclusions Our findings show that a classifier combining histopathological and molecular factors outperforms conventional methods for prognosticating clinical outcome in patients with OPMD. We have also shown that formalin-fixed paraffin-embedded tissue can be used to generate a molecular classification with clinical utility.

Published

2019

12. Scx+/Sox9+ progenitors contribute to the establishment of the junction between cartilage and tendon/ligament

Author

Gerd Scherer, Takashi Nakamura, Yuki Sugimoto, Ralf Kist, Yuji Hiraki, Chisa Shukunami, Haruhiko Akiyama, and Aki Takimoto

Subjects

endocrine system, animal structures, Population, Mice, Transgenic, SOX9, Biology, Bone and Bones, Mesoderm, Tendons, Mice, stomatognathic system, Basic Helix-Loop-Helix Transcription Factors, medicine, Animals, Progenitor cell, education, Molecular Biology, Progenitor, education.field_of_study, Ligaments, Stem Cells, Cartilage, Scleraxis, Gene Expression Regulation, Developmental, SOX9 Transcription Factor, Tendon formation, Anatomy, musculoskeletal system, Tendon, Cell biology, medicine.anatomical_structure, embryonic structures, Developmental Biology

Abstract

SRY-box containing gene 9 (Sox9) and scleraxis (Scx) regulate cartilage and tendon formation, respectively. Here we report that murine Scx(+)/Sox9(+) progenitors differentiate into chondrocytes and tenocytes/ligamentocytes to form the junction between cartilage and tendon/ligament. Sox9 lineage tracing in the Scx(+) domain revealed that Scx(+) progenitors can be subdivided into two distinct populations with regard to their Sox9 expression history: Scx(+)/Sox9(+) and Scx(+)/Sox9(-) progenitors. Tenocytes are derived from Scx(+)/Sox9(+) and Scx(+)/Sox9(-) progenitors. The closer the tendon is to the cartilaginous primordium, the more tenocytes arise from Scx(+)/Sox9(+) progenitors. Ligamentocytes as well as the annulus fibrosus cells of the intervertebral discs are descendants of Scx(+)/Sox9(+) progenitors. Conditional inactivation of Sox9 in Scx(+)/Sox9(+) cells causes defective formation in the attachment sites of tendons/ligaments into the cartilage, and in the annulus fibrosus of the intervertebral discs. Thus, the Scx(+)/Sox9(+) progenitor pool is a unique multipotent cell population that gives rise to tenocytes, ligamentocytes and chondrocytes for the establishment of the chondro-tendinous/ligamentous junction.

Published

2013

13. E-cigarettes and oral health: a balanced viewpoint

Author

Linda Bauld, Richard Holliday, Ralf Kist, and Philip M. Preshaw

Subjects

03 medical and health sciences, medicine.medical_specialty, 0302 clinical medicine, Otorhinolaryngology, business.industry, 030220 oncology & carcinogenesis, Family medicine, MEDLINE, Medicine, 030206 dentistry, Oral health, business, General Dentistry

Published

2017

14. Mice Lacking Ly49E Show Normal NK Cell Development and Provide Evidence for Probabilistic Expression of Ly49E in NK Cells and T Cells

Author

Heiko Peters, Jonathan G. Aust, Colin G. Brooks, Ralf Kist, Farhana Hussain, Geoffrey W. Butcher, and Frances Gays

Subjects

Male, T-Lymphocytes, Cellular differentiation, T cell, Immunology, CD1, Mice, Transgenic, Mice, Interleukin 21, MHC class I, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Gene Knock-In Techniques, Cells, Cultured, Cellular Senescence, Mice, Knockout, biology, Cell Differentiation, Natural killer T cell, Molecular biology, Killer Cells, Natural, Mice, Inbred C57BL, medicine.anatomical_structure, Gene Expression Regulation, biology.protein, Interleukin 12, NK Cell Lectin-Like Receptor Subfamily A

Abstract

Ly49E is an unusual member of the Ly49 family that is expressed on fetal NK cells, epithelial T cells, and NKT cells, but not on resting adult NK cells. Ly49Ebgeo/bgeo mice in which the Ly49E gene was disrupted by inserting a β-geo transgene were healthy, fertile, and had normal numbers of NK and T cells in all organs examined. Their NK cells displayed normal expression of Ly49 and other NK cell receptors, killed tumor and MHC class I-deficient cells efficiently, and produced normal levels of IFN-γ. In heterozygous Ly49E+/bgeo mice, the proportion of epidermal T cells, NKT cells, and IL-2–activated NK cells that expressed Ly49E was about half that found in wild-type mice. Surprisingly, although splenic T cells rarely expressed Ly49E, IL-2–activated splenic T cells from Ly49Ebgeo/bgeo mice were as resistant to growth in G418 as NK cells and expressed similar levels of β-geo transcripts, suggesting that disruption of the Ly49E locus had increased its expression in these cells to the same level as that in NK cells. Importantly, however, the proportion of G418-resistant heterozygous Ly49E+/bgeo cells that expressed Ly49E from the wild-type allele was similar to that observed in control cells. Collectively, these findings demonstrate that Ly49E is not required for the development or homeostasis of NK and T cell populations or for the acquisition of functional competence in NK cells and provide compelling evidence that Ly49E is expressed in a probabilistic manner in adult NK cells and T cells.

Published

2011

15. Abstract 4471: Pax9 regulates squamous cell differentiation and alcohol-associated carcinogenesis in the oro-esophageal epithelium

Author

Xiaoxin Luke Chen, Zheng Sun, Hao Chen, Yawan Lyvia Zhang, Zhaohui Xiong, Shuang Ren, Katherine S. Garman, Heiko Peters, Joab Otieno Odera, Tong Chen, Ralf Kist, Caizhi Huang, and Yao Liu

Subjects

Cancer Research, Cell growth, Cellular differentiation, Cell, Cancer, Biology, medicine.disease, medicine.disease_cause, Epithelium, stomatognathic diseases, medicine.anatomical_structure, Oncology, medicine, Cancer research, Esophagus, Carcinogenesis, PAX9

Abstract

Pax9 is a transcription factor of the Pax family characterized by a DNA-binding paired domain. Previous studies have suggested a potential role of Pax9 in squamous cell differentiation and carcinogenesis of oro-esophageal epithelium. However, its functional role in differentiation and carcinogenesis remains unclear. In this study, Pax9 deficiency in mouse esophagus promoted cell proliferation, delayed cell differentiation and altered the global gene expression profile. Ethanol exposure down-regulated Pax9 expression in human esophageal epithelial cells in vitro and mouse forestomach and tongue in vivo. We further showed that PAX9 was down-regulated in human oro-esophageal squamous cell carcinoma (OESCC), and its down-regulation was associated with alcohol drinking and promoter hypermethylation. Moreover, ad libitum feeding with an isocaloric Lieber-DeCarli liquid diet containing ethanol for 40 weeks or Pax9 deficiency promoted NMBA-induced squamous cell carcinogenesis in mouse tongue, esophagus, and forestomach. In conclusion, Pax9 regulates squamous cell differentiation in the oro-esophageal epithelium. Alcohol drinking and promoter hypermethylation are associated with PAX9 silencing in human OESCC. Pax9 down-regulation, at least in part, contributes to alcohol-associated oro-esophageal squamous cell carcinogenesis. Citation Format: Zhaohui Xiong, Shuang Ren, Hao Chen, Yao Liu, Caizhi Huang, Yawan Lyvia Zhang, Joab Otieno Odera, Tong Chen, Ralf Kist, Heiko Peters, Katherine Garman, Zheng Sun, Xiaoxin Luke Chen. Pax9 regulates squamous cell differentiation and alcohol-associated carcinogenesis in the oro-esophageal epithelium [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 4471.

Published

2018

16. Genetic interactions between Pax9 and Msx1 regulate lip development and several stages of tooth morphogenesis

Author

Jennifer J. Lund, Richard L. Maas, Annick Turbe-Doan, YiPing Chen, Xiu-Ping Wang, Heiko Peters, Mitsushiro Nakatomi, Andrew Aw, Ralf Kist, and Darren Key

Subjects

Oligodontia, Fgf3, Mutant, Cervical loop, Mice, 0302 clinical medicine, Morphogenesis, Paired Box Transcription Factors, In Situ Hybridization, Mice, Knockout, Genetics, 0303 health sciences, Gene Expression Regulation, Developmental, Immunohistochemistry, Phenotype, Cell biology, Incisor, medicine.anatomical_structure, Odontogenesis, Heterozygote, Transgene, Mesenchyme, Bmp4, Mice, Inbred Strains, Biology, Tooth development, 03 medical and health sciences, stomatognathic system, medicine, Animals, Molecular Biology, 030304 developmental biology, MSX1 Transcription Factor, FGF10, Fgf10, Cleft lip, 030206 dentistry, Cell Biology, Pax9, Embryo, Mammalian, Lip, Mice, Inbred C57BL, stomatognathic diseases, Ameloblast differentiation, Mice, Inbred CBA, PAX9 Transcription Factor, Tooth, PAX9, Msx1, Developmental Biology

Abstract

Developmental abnormalities of craniofacial structures and teeth often occur sporadically and the underlying genetic defects are not well understood, in part due to unknown gene–gene interactions. Pax9 and Msx1 are co-expressed during craniofacial development, and mice that are single homozygous mutant for either gene exhibit cleft palate and an early arrest of tooth formation. Whereas in vitro assays have demonstrated that protein–protein interactions between Pax9 and Msx1 can occur, it is unclear if Pax9 and Msx1 interact genetically in vivo during development. To address this question, we compounded the Pax9 and Msx1 mutations and observed that double homozygous mutants exhibit an incompletely penetrant cleft lip phenotype. Moreover, in double heterozygous mutants, the lower incisors were consistently missing and we find that transgenic BMP4 expression partly rescues this phenotype. Reduced expression of Shh and Bmp2 indicates that a smaller “incisor field” forms in Pax9+/−;Msx1+/− mutants, and dental epithelial growth is substantially reduced after the bud to cap stage transition. This defect is preceded by drastically reduced mesenchymal expression of Fgf3 and Fgf10, two genes that encode known stimulators of epithelial growth during odontogenesis. Consistent with this result, cell proliferation is reduced in both the dental epithelium and mesenchyme of double heterozygous mutants. Furthermore, the developing incisors lack mesenchymal Notch1 expression at the bud stage and exhibit abnormal ameloblast differentiation on both labial and lingual surfaces. Thus, Msx1 and Pax9 interact synergistically throughout lower incisor development and affect multiple signaling pathways that influence incisor size and symmetry. The data also suggest that a combined reduction of PAX9 and MSX1 gene dosage in humans may increase the risk for orofacial clefting and oligodontia.

Published

2010

17. Loss of Sox9 function results in defective chondrocyte differentiation of mouse embryonic stem cells in vitro

Author

Ralf Kist, Daniela Gerstel, Jan Kramer, Jürgen Rohwedel, Gunnar Hargus, Gerd Scherer, and Angela Neitz

Subjects

endocrine system, Embryology, animal structures, Cellular differentiation, Molecular Sequence Data, Biology, Chondrocyte, Mice, Limb bud, Chondrocytes, stomatognathic system, medicine, Animals, Amino Acid Sequence, Collagen Type II, Embryonic Stem Cells, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, Cartilage, Scleraxis, Mesenchymal stem cell, High Mobility Group Proteins, Gene Expression Regulation, Developmental, Cell Differentiation, SOX9 Transcription Factor, DNA, Exons, musculoskeletal system, Chondrogenesis, Embryonic stem cell, Clone Cells, Cell biology, medicine.anatomical_structure, Gene Targeting, embryonic structures, Immunology, Transcription Factors, Developmental Biology

Abstract

The transcription factor Sox9 plays an important role during chondrogenesis. After early conditional inactivation of Sox9 in mesenchymal limb bud cells of mice, mesenchymal condensations as well as cartilage and bone are completely absent in the developing limbs. We analyzed chondrogenic differentiation of Sox9-/- mouse embryonic stem cells in vitro, using two clones with different targeted mutations. We found that the development of mature and hypertrophic chondrocytes is completely inhibited in the absence of Sox9 confirming that Sox9 is required for the formation of cartilage. In contrast, Sox9+/- mouse embryonic stem cells showed continuous but reduced differentiation into mature chondrocytes. Interestingly, the formation of early chondrogenic condensations expressing characteristic marker genes such as scleraxis, Sox5 and Sox6 was not inhibited in the absence of Sox9 in vitro. Thus, we propose that the earliest step of chondrogenesis could be regulated by a non cell-autonomous function of Sox9.

Published

2008

18. Homozygous Inactivation of Sox9 Causes Complete XY Sex Reversal in Mice1

Author

Francisco J. Barrionuevo, Christoph Englert, Makoto Mark Taketo, Gerd Scherer, Stefan Bagheri-Fam, Ralf Kist, and Jürgen Klattig

Subjects

endocrine system, medicine.medical_specialty, animal structures, Gonad, Cre recombinase, Cell Biology, General Medicine, SOX9, Sex reversal, Biology, Sertoli cell, Cell biology, medicine.anatomical_structure, Endocrinology, Testis determining factor, stomatognathic system, Reproductive Medicine, Internal medicine, embryonic structures, WNT4, Primary sex determination, medicine

Abstract

In the presence of the Y-chromosomal gene Sry, the bipotential mouse gonads develop as testes rather than as ovaries. The autosomal gene Sox9, a likely and possibly direct Sry target, can induce testis development in the absence of Sry. Sox9 is thus sufficient but not necessarily essential for testis induction. Mutational inactivation of one allele of SOX9/Sox9 causes sex reversal in humans but not in mice. Because Sox9 –/– embryos die around Embryonic Day 11.5 (E11.5) at the onset of testicular morphogenesis, differentiation of the mutant XY gonad can be analyzed only ex vivo in organ culture. We have therefore conditionally inactivated both Sox9 alleles in the gonadal anlagen using the CRE/loxP recombination system, whereby CRE recombinase is under control of the cytokeratin 19 promoter. Analysis of resulting Sox9 –/– XY gonads up to E15.5 reveals immediate, complete sex reversal, as shown by expression of the early ovary-specific markers Wnt4 and Foxl2 and by lack of testis cord and Leydig cell formation. Sry expression in mutant XY gonads indicates that downregulation of Wnt4 and Foxl2 is dependent on Sox9 rather than on Sry. Our results provide in vivo proof that, in contrast to the situation in humans, complete XY sex reversal in mice requires inactivation of both Sox9 alleles and that Sox9 is essential for testogenesis in mice. developmental biology, gene regulation, ovary, Sertoli cells, testis

Published

2006

19. Normal lung development and function afterSox9 inactivation in the respiratory epithelium

Author

Zhengyuan Shan, Gerd Scherer, Anne-Karina T. Perl, Jeffrey A. Whitsett, and Ralf Kist

Subjects

Transcriptional Activation, Pathology, medicine.medical_specialty, Time Factors, animal structures, Organogenesis, Morphogenesis, Mice, Transgenic, Respiratory Mucosa, SOX9, Biology, Mice, Endocrinology, stomatognathic system, Pregnancy, Genetics, medicine, Animals, Respiratory system, Lung, Crosses, Genetic, Respiratory distress, High Mobility Group Proteins, Cell Biology, respiratory system, medicine.disease, Immunohistochemistry, Mice, Mutant Strains, respiratory tract diseases, Campomelic dysplasia, medicine.anatomical_structure, Doxycycline, embryonic structures, Immunology, RNA, Respiratory epithelium, Female, Lung morphogenesis, Gene Deletion, Transcription Factors

Abstract

Heterozygous mutations in the human SOX9 gene cause campomelic dysplasia (CD), a skeletal malformation syndrome with various other organ defects. Severely affected CD patients usually die in the neonatal period due to respiratory distress. We analyzed the dynamic expression pattern of Sox9 in the developing mouse lung throughout morphogenesis. To determine a role of Sox9 in lung development and function, Sox9 was specifically inactivated in respiratory epithelial cells of the mouse lung using a doxycycline-inducible Cre/loxP system. Immunohistochemical and RNA analysis demonstrated extensive inactivation of Sox9 in the embryonic stage of lung development as early as embryonic day (E) 12.5. Lung morphogenesis and lung function after birth were not altered. Compensatory upregulation of Sox2, Sox4, Sox8, Sox10, Sox11, and Sox17 was not detected. Although Sox9 is expressed at high levels throughout lung morphogenesis, inactivation of Sox9 from the respiratory epithelial cells does not alter lung structure, postnatal survival, or repair following oxygen injury.

Published

2005

20. Pax9 is required for filiform papilla development and suppresses skin-specific differentiation of the mammalian tongue epithelium

Author

Heiko Peters, Ralf Kist, Andrew Aw, Ilka Wappler, and Leon Jonker

Subjects

Embryology, Cellular differentiation, Down-Regulation, Biology, Epithelium, Mice, Tongue, Cell polarity, Keratin, medicine, Animals, Paired Box Transcription Factors, Lingual papilla, Oligonucleotide Array Sequence Analysis, Skin, Homeodomain Proteins, chemistry.chemical_classification, integumentary system, Gene Expression Profiling, Cell Polarity, Gene Expression Regulation, Developmental, Cell Differentiation, Anatomy, Surface ectoderm, Mice, Mutant Strains, Cell biology, stomatognathic diseases, medicine.anatomical_structure, Epidermis (zoology), chemistry, Mutation, Keratins, PAX9 Transcription Factor, Transcription Factors, Developmental Biology

Abstract

The epidermis is a derivative of the surface ectoderm. It forms a protective barrier and specific appendages including hair, nails, and different eccrine glands. The surface ectoderm also forms the epithelium of the oral cavity and tongue, which develop a slightly different barrier and form different appendages such as teeth, filiform papillae, taste papillae, and salivary glands. How this region-specific differentiation is genetically controlled is largely unknown. We show here that Pax9, which is expressed in the epithelium of the tongue but not in skin, regulates several aspects of tongue-specific epithelial differentiation. In Pax9-deficient mice filiform papillae lack the anterior-posterior polarity, a defect that is associated with temporal-spatial changes in Hoxc13 expression. Barrier formation is disturbed in the mutant tongue and genome-wide expression profiling revealed that the expression of specific keratins (Krt), keratin-associated proteins, and members of the epidermal differentiation complex is significantly down-regulated. In situ hybridization demonstrated that several 'hard' keratins, Krt1-5, Krt1-24, and Krt2-16, are not expressed in the absence of Pax9. Notably, specific 'soft' keratins, Krt2-1 and Krt2-17, normally weakly expressed in the tongue but present at high levels in skin and in orthokeratinized oral dysplasia are up-regulated in the mutant tongue epithelium. This result indicates a partial trans-differentiation to an epithelium with skin-specific characteristics. Together, our findings show that Pax9 regulates appendage formation in the mammalian tongue and identify Pax9 as an important factor for the region-specific differentiation of the surface ectoderm.

Published

2004

21. E-cigarette vapour is not inert and exposure can lead to cell damage

Author

Linda Bauld, Ralf Kist, and Richard Holliday

Subjects

DNA damage, business.industry, medicine.disease, medicine.disease_cause, Head and neck squamous-cell carcinoma, Molecular biology, Toxicology, Comet assay, 03 medical and health sciences, HaCaT, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, 030212 general & internal medicine, Viability assay, Clonogenic assay, business, General Dentistry, Cell damage, Genotoxicity

Abstract

In vitro experiments were performed on normal epithelial cells as well as head and neck squamous cell carcinoma (HNSCC) cell lines. The widely available cell line HaCat, a spontaneously transformed immortal keratinocyte and the HNSCC cell lines HN30 and UMSCC10B were used. Cells were exposed to nicotine-containing and nicotine-free vapour extract from two popular e-cigarette brands for periods ranging from 48 hours to eight weeks. Cytotoxicity was assessed using Annexin V flow cytometric analysis, trypan blue exclusion and clonogenic assays. Genotoxicity in the form of DNA strand breaks was quantified using the neutral comet assay and γ-H2AX immunostaining. E-cigarette-exposed cells showed significantly reduced cell viability and clonogenic survival, along with increased rates of apoptosis and necrosis, regardless of e-cigarette vapour nicotine content. They also exhibited significantly increased comet tail length and accumulation of γ-H2AX foci, demonstrating increased DNA strand breaks. In conclusion, our study strongly suggests that electronic cigarettes are not as safe as their marketing makes them appear to the public. Our in vitro experiments employing two brands of e-cigs show that at biologically relevant doses, vapourised e-cig liquids induce increased DNA strand breaks and cell death, and decreased clono- genic survival in both normal epithelial and HNSCC cell lines independently of nicotine content. Further research is needed to definitively determine the long-term effects of e-cig usage, as well as whether the DNA damage shown in our study as a result of e-cig exposure will lead to mutations that ultimately result in cancer.

Published

2016

22. Transcription factor SOX9 plays a key role in the regulation of visual cycle gene expression in the retinal pigment epithelium

Author

Tomohiro Masuda, Joshua L. Dunaief, Karl J. Wahlin, Natalie Wolkow, Jiang Qian, Jun Wan, Jared Iacovelli, Donald J. Zack, Ralf Kist, Noriko Esumi, Julien Maruotti, Jianfei Hu, and Xue Yang

Subjects

cis-trans-Isomerases, genetic structures, LIM-Homeodomain Proteins, Retinal Pigment Epithelium, Biology, Biochemistry, Cell Line, Mice, medicine, Animals, Humans, Gene Regulatory Networks, Gene Regulation, Eye Proteins, Molecular Biology, Transcription factor, Orthodenticle homeobox 2, Cells, Cultured, Regulation of gene expression, Mice, Knockout, Retinal pigment epithelium, Binding Sites, Otx Transcription Factors, Models, Genetic, Reverse Transcriptase Polymerase Chain Reaction, Promoter, SOX9 Transcription Factor, Cell Biology, Molecular biology, Immunohistochemistry, eye diseases, Chromatin, MicroRNAs, medicine.anatomical_structure, HEK293 Cells, RPE65, Gene Expression Regulation, Cis-trans-Isomerases, embryonic structures, sense organs, Carrier Proteins, Visual phototransduction, Transcription Factors

Abstract

The retinal pigment epithelium (RPE) performs specialized functions to support retinal photoreceptors, including regeneration of the visual chromophore. Enzymes and carrier proteins in the visual cycle function sequentially to regenerate and continuously supply 11-cis-retinal to retinal photoreceptor cells. However, it is unknown how the expression of the visual cycle genes is coordinated at the transcriptional level. Here, we show that the proximal upstream regions of six visual cycle genes contain chromatin-accessible sex-determining region Y box (SOX) binding sites, that SOX9 and LIM homeobox 2 (LHX2) are coexpressed in the nuclei of mature RPE cells, and that SOX9 acts synergistically with orthodenticle homeobox 2 (OTX2) to activate the RPE65 and retinaldehyde binding protein 1 (RLBP1) promoters and acts synergistically with LHX2 to activate the retinal G protein-coupled receptor (RGR) promoter. ChIP reveals that SOX9 and OTX2 bind to the promoter regions of RPE65, RLBP1, and RGR and that LHX2 binds to those of RPE65 and RGR in bovine RPE. ChIP with human fetal RPE cells shows that SOX9 and OTX2 also bind to the human RPE65, RLBP1, and RGR promoters. Conditional inactivation of Sox9 in mouse RPE results in reduced expression of several visual cycle genes, most dramatically Rpe65 and Rgr. Furthermore, bioinformatic analysis predicts that multiple common microRNAs (miRNAs) regulate visual cycle genes, and cotransfection of miRNA mimics with luciferase reporter constructs validated some of the predicted miRNAs. These results implicate SOX9 as a key regulator of visual cycle genes, reveal for the first time the functional role of LHX2 in the RPE, and suggest the possible regulation of visual cycle genes by common miRNAs.

Published

2014

23. Conditional inactivation ofSox9: A mouse model for campomelic dysplasia

Author

Ralf Kist, Rudi Balling, Heinrich Schrewe, and Gerd Scherer

Subjects

endocrine system, Mutant, Cre recombinase, Mice, Transgenic, SOX9, Biology, Mice, Exon, Endocrinology, stomatognathic system, Genetics, medicine, Animals, Phenocopy, Bone Diseases, Developmental, High Mobility Group Proteins, Gene targeting, SOX9 Transcription Factor, Cell Biology, musculoskeletal system, medicine.disease, Null allele, Molecular biology, Campomelic dysplasia, Disease Models, Animal, Gene Expression Regulation, embryonic structures, Transcription Factors

Abstract

Campomelic dysplasia (CD), a semilethal human skeletal malformation syndrome with XY sex reversal, is caused by heterozygous mutations in the SRY-related transcription factor gene SOX9 (Foster et al., 1994; Wagner et al., 1994). The mouse Sox9 gene, located on distal chromosome 11, is expressed during chondrogenesis (Wright et al., 1995), and is a key regulator of cartilage differentiation (Bi et al., 1999) and testis development (Vidal et al., 2001). Sox9 is expressed in a variety of embryonic tissues (Ng et al., 1997), suggesting further functions for Sox9/SOX9 during organogenesis. Indeed, CD patients show malformations in nonskeletal organs such as brain, heart, and kidneys (Houston et al., 1983; Mansour et al., 1995). Recently, Sox9 / mutant mice have been generated by a classical gene targeting approach and were shown to phenocopy the skeletal malformations observed in CD (Bi et al., 2001). However, because Sox9 / mice die shortly after birth, it was not possible to generate a stable Sox9 mutant mouse line. To circumvent this problem and to provide a tool for an in-depth analysis of Sox9 functions in skeletal development and the formation of other organs, we have generated a conditional Sox9 mutant allele in mice using the Cre/loxP system (Nagy, 2000; Le and Sauer, 2001) (Fig.1). Five correctly targeted embryonic stem (ES) cell clones were identified, and, following successful deletion of the neo cassette by transient in vitro expression of Cre recombinase (Taniguchi et al., 1998), two clones were microinjected into C57BL/6 blastocysts. Germline transmission was obtained for both clones and two Sox9-flox mouse lines have been established by backcrossing to C57BL/6 mice. Both Sox9 homozygous male and female mice are viable and fertile and do not show any obvious phenotype. To test for conditional inactivation of Sox9 in vivo, Sox9 /flox mice were crossed to Cre deleter mice which ubiquitously express the Cre recombinase (Schwenk et al., 1995) (Fig 2a). In Sox9 ; Cre–transgenic animals, designated as Sox9 / , exon 2 encoding half of the DNA-binding high-mobility group (HMG) domain and exon 3 encoding the entire transactivation domain are deleted (Fig. 2a, b). Because the transactivation domain is essential for SOX9 function (Sudbeck et al., 1996), and because truncated HMG domains cannot bind to DNA (Giese et al., 1991), our strategy most likely results in a functional null allele of the Sox9 gene. Complete recombination of the loxP-flanked Sox9 allele was demonstrated by allele-specific PCR analysis of Sox9 / mutants (Fig. 2c). Sox9 / mice died shortly after birth, presumably because of severe respiratory failure caused by a cleft secondary palate. Skeletal staining of newborn Sox9 / mutants revealed bone malformations typically observed in CD patients (Fig. 2 and data not shown). For example, the scapula was hypoplastic and malformed and the deltoid tuberosity of the humerus was missing (Fig. 2e). In addition, premature mineralization occurred in many skeletal elements, including the tail vertebrae (Fig. 2g). This is in agreement with the recently proposed role for Sox9 in regulating the rate of hypertrophic chondrocyte differentiation (Bi et al., 2001). Taken together, our analysis revealed that the skeletal phenotype of conditional Sox9 / mutants is very similar to that described for Sox9 / mutants (Bi et al., 2001). The different genetic background of mice used in the two studies may account for minor differences we observed in the severity of the skeletal phenotypes. The availability of tissue-specific or inducible Cre-transgenic mouse strains will make the conditional Sox9 allele a valuable tool not only to understand cartilage differentiation and skeletogenesis but also to investigate Sox9 functions during the development of a variety of other organs during mammalian development.

Published

2002

24. Hydroureternephrosis due to loss of Sox9-regulated smooth muscle cell differentiation of the ureteric mesenchyme

Author

Marianne Petry, Andreas Kispert, Karin Schuster-Gossler, Michaela Schweizer, Mark-Oliver Trowe, Gerd Scherer, Henner F. Farin, Anna B. Foik, Ralf Kist, and Rannar Airik

Subjects

medicine.medical_specialty, Mesenchyme, Smooth muscle cell differentiation, Cellular differentiation, Myocytes, Smooth Muscle, SOX9, Hydronephrosis, Biology, Hydroureter, Kidney, Extracellular matrix, Mesoderm, Mice, Internal medicine, Genetics, medicine, Animals, Gene Silencing, Molecular Biology, Genetics (clinical), Kidney metabolism, Gene Expression Regulation, Developmental, Cell Differentiation, SOX9 Transcription Factor, General Medicine, musculoskeletal system, medicine.disease, Embryo, Mammalian, Cell biology, Extracellular Matrix, Campomelic dysplasia, medicine.anatomical_structure, Endocrinology, Mutation, Ureter

Abstract

Congenital ureter anomalies, including hydroureter, affect up to 1% of the newborn children. Despite the prevalence of these developmental abnormalities in young children, the underlying molecular causes are only poorly understood. Here, we show that the high mobility group domain transcription factor Sox9 plays an important role in ureter development in the mouse. Transient Sox9 expression was detected in the undifferentiated ureteric mesenchyme and inactivation of Sox9 in this domain resulted in strong proximal hydroureter formation due to functional obstruction. Loss of Sox9 did not affect condensation, proliferation and apoptosis of the undifferentiated mesenchyme, but perturbed cyto-differentiation into smooth muscle cells (SMCs). Expression of genes encoding extracellular matrix (ECM) components was strongly reduced, suggesting that deficiency in ECM composition and/or signaling may underlie the observed defects. Prolonged expression of Sox9 in the ureteric mesenchyme led to increased deposition of ECM components and SMC dispersal. Furthermore, Sox9 genetically interacts with the T-box transcription factor 18 gene (Tbx18) during ureter development at two levels--as a downstream mediator of Tbx18 function and in a converging pathway. Together, our results argue that obstructive uropathies in campomelic dysplasia patients that are heterozygous for mutations in and around SOX9 arise from a primary requirement of Sox9 in the development of the ureteric mesenchyme.

Published

2010

25. Loss of Sox9 in the periotic mesenchyme affects mesenchymal expansion and differentiation, and epithelial morphogenesis during cochlea development in the mouse

Author

Ralf Kist, Karin Schuster-Gossler, Marianne Petry, Andreas Kispert, Rannar Airik, Mark-Oliver Trowe, and Sadrick Shah

Subjects

endocrine system, animal structures, Mesenchyme, Otic capsule, Morphogenesis, Otic placode formation, Cochlear duct, Mice, Transgenic, Biology, Epithelium, Mesoderm, Mice, stomatognathic system, Fibrocyte, Inner ear, medicine, Compartment (development), Animals, Otic placode, Molecular Biology, Cell Differentiation, Ear, SOX9 Transcription Factor, Anatomy, Cell Biology, Chondrogenesis, Cell biology, Cochlea, medicine.anatomical_structure, Epithelial–mesenchymal interaction, Ear, Inner, embryonic structures, Otic fibrocytes, sense organs, Periotic mesenchyme, Developmental Biology, Signal Transduction

Abstract

Sox9 encodes an HMG-domain transcription factor that is critically required in numerous developmental processes such as chondrogenesis and otic placode formation. Here, we show that Sox9 is expressed in the mesenchyme surrounding the developing cochlea in the mouse suggesting that Sox9 may also control development of the otic fibrocyte compartment and the surrounding otic capsule. Tissue-specific inactivation of Sox9 in the periotic mesenchyme using a Tbx18Cre mouse line results in arrest of early chondrogenesis and consequently, in a lack of cochlear otic capsule formation. Furthermore, loss of Sox9 severely compromises expansion, differentiation and remodeling of the otic fibrocyte compartment. Early cell proliferation defects in the entire periotic mesenchyme of Sox9-deficient inner ears suggest a cell-autonomous function of Sox9 for the development of the inner mesenchymal compartment. Abnormal cochlear duct morphogenesis in Sox9 mutants including disruption of the coiling process is tightly associated with the onset of mesenchymal defects whereas the absence of major differentiation defects in the otic epithelium suggests that Sox9-dependent mesenchymal signals primarily control epithelial morphogenesis.

Published

2009

26. Haploinsufficiency of the germ cell-specific nuclear RNA binding protein hnRNP G-T prevents functional spermatogenesis in the mouse

Author

Aikaterini Tsaousi, Philippa T. K. Saunders, David J. Elliott, Michael J. Mitchell, Bettina Heinrich, Ingrid Ehrmann, Christian Mueller, Karim Nayernia, Maria Paola Paronetto, Caroline Dalgliesh, Michael S. Jackson, Heiko Peters, Claudio Sette, Paul Cairns, Stefan Stamm, Ralf Kist, and Weiping Li

Subjects

Male, Molecular Sequence Data, Mice, Inbred Strains, Biology, Haploidy, Heterogeneous-Nuclear Ribonucleoproteins, Mice, Meiosis, Genetics, medicine, Animals, Humans, Amino Acid Sequence, Nuclear protein, Selection, Genetic, Spermatogenesis, Molecular Biology, Gene, Genetics (clinical), Embryonic Stem Cells, Infertility, Male, Phylogeny, Mammals, Settore BIO/16, Chimera, General Medicine, Sperm, Spermatozoa, Cell biology, medicine.anatomical_structure, Germ line development, Haploinsufficiency, Sequence Alignment, Germ cell

Abstract

Human HNRNPGT, encoding the protein hnRNP G-T, is one of several autosomal retrogenes derived from RBMX. It has been suggested that HNRNPGT functionally replaces the sex-linked RBMX and RBMY genes during male meiosis. We show here that during normal mouse germ cell development, hnRNP G-T protein is strongly expressed during and after meiosis when proteins expressed from Rbmx or Rbmx-like genes are absent. Amongst these Rbmx-like genes, DNA sequence analyses indicate that two other mouse autosomal Rbmx-derived retrogenes have evolved recently in rodents and one already shows signs of degenerating into a non-expressed pseudogene. In contrast, orthologues of Hnrnpgt are present in all four major groups of placental mammals. The sequence of Hnrnpgt is under considerable positive selection suggesting it performs an important germ cell function in eutherians. To test this, we inactivated Hnrnpgt in ES cells and studied its function during spermatogenesis in chimaeric mice. Although germ cells heterozygous for this targeted allele could produce sperm, they did not contribute to the next generation. Chimaeric mice with a high level of mutant germ cells were infertile with low sperm counts and a high frequency of degenerate seminiferous tubules and abnormal sperm. Chimaeras made from a 1:1 mix of targeted and wild-type ES cell clones transmitted wild-type germ cells only. Our data show that haploinsufficiency of Hnrnpgt results in abnormal sperm production in the mouse. Genetic defects resulting in reduced levels of HNRNPGT could, therefore, be a cause of male infertility in humans.

Published

2008

27. Sox9 regulates cell proliferation and is required for Paneth cell differentiation in the intestinal epithelium

Author

Pauline Bastide, Gerd Scherer, Frédéric Bibeau, Charbel Darido, Frédéric Hollande, Christiane Marty-Double, Philippe Blache, Julie Pannequin, Dominique Joubert, Sylvie Robine, Ralf Kist, Philippe Jay, Institut de Génomique Fonctionnelle (IGF), Université de Montpellier (UM)-Université Montpellier 1 (UM1)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Montpellier 2 - Sciences et Techniques (UM2)-Centre National de la Recherche Scientifique (CNRS), Institute of Human Genetics and Anthropology, University of Freiburg [Freiburg], Morphogénèse et Signalisation Cellulaires, Institut Curie [Paris]-Centre National de la Recherche Scientifique (CNRS), Service d'anatomie-pathologie, Hôpital Universitaire Carémeau [Nîmes] (CHU Nîmes), Centre Hospitalier Universitaire de Nîmes (CHU Nîmes)-Centre Hospitalier Universitaire de Nîmes (CHU Nîmes), Laboratoire d'anatomo-pathologie, CRLCC Val d'Aurelle - Paul Lamarque, This work has been supported by Agence Nationale pour la Recherche (Jeune Chercheur), Association pour la Recherche contre le Cancer (ARC N°3570 and 3636), Ligue Nationale contre le Cancer (Equipe Labellisée), Fondation pour la Recherche Médicale and Groupement des Entreprises Françaises dans la Lutte contre le Cancer (GEFLUC). C.D. is supported by a CNRS-L fellowship. G.S. acknowledges support through grant Sche 194/15-1 and -2 by the Deutsche Forschungsgemeinschaft., Jay, Philippe, and Université Montpellier 1 (UM1)-Université Montpellier 2 - Sciences et Techniques (UM2)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects

[SDV.GEN] Life Sciences [q-bio]/Genetics, Mice, 0302 clinical medicine, MESH: Animals, Research Articles, 0303 health sciences, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, Wnt signaling pathway, High Mobility Group Proteins, Cell Differentiation, SOX9 Transcription Factor, differentiation, MESH: Transcription Factors, Intestinal epithelium, Cell biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Sox9, MESH: Cell Differentiation, Paneth Cells, MESH: Cell Line, Tumor, Colon, [SDV.CAN]Life Sciences [q-bio]/Cancer, SOX9, Biology, Article, 03 medical and health sciences, Wnt, [SDV.CAN] Life Sciences [q-bio]/Cancer, MESH: Mice, Inbred C57BL, MESH: Cell Proliferation, Cell Line, Tumor, medicine, Animals, Humans, Progenitor cell, MESH: Colon, Transcription factor, intestine, MESH: Mice, 030304 developmental biology, Cell Proliferation, Goblet cell, [SDV.GEN]Life Sciences [q-bio]/Genetics, MESH: Humans, MESH: Paneth Cells, Cell growth, Cell Biology, MESH: High Mobility Group Proteins, Mice, Inbred C57BL, Paneth cell, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, Transcription Factors

Abstract

International audience; The HMG-box transcription factor Sox9 is expressed in the intestinal epithelium, specifically, in stem/progenitor cells and in Paneth cells. Sox9 expression requires an active beta-catenin-Tcf complex, the transcriptional effector of the Wnt pathway. This pathway is critical for numerous aspects of the intestinal epithelium physiopathology, but processes that specify the cell response to such multipotential signals still remain to be identified. We inactivated the Sox9 gene in the intestinal epithelium to analyze its physiological function. Sox9 inactivation affected differentiation throughout the intestinal epithelium, with a disappearance of Paneth cells and a decrease of the goblet cell lineage. Additionally, the morphology of the colon epithelium was severely altered. We detected general hyperplasia and local crypt dysplasia in the intestine, and Wnt pathway target genes were up-regulated. These results highlight the central position of Sox9 as both a transcriptional target and a regulator of the Wnt pathway in the regulation of intestinal epithelium homeostasis.

Published

2007

28. SOX9 is required for maintenance of the pancreatic progenitor cell pool

Author

Ralf Kist, Jan Jensen, Kristine K. Freude, Erin Mayes, Maike Sander, Philip A. Seymour, Gerd Scherer, and Man N. Tran

Subjects

Pluripotent Stem Cells, endocrine system, Cell Survival, Cellular differentiation, Pancreas morphogenesis, Mice, Transgenic, Biology, Mice, medicine, Animals, Progenitor cell, HES1, Induced pluripotent stem cell, Pancreas, Cell Proliferation, Mice, Knockout, Multidisciplinary, High Mobility Group Proteins, Cell Differentiation, SOX9 Transcription Factor, Biological Sciences, medicine.anatomical_structure, embryonic structures, Cancer research, Pancreatic progenitor cell, PDX1, Female, Signal Transduction, Transcription Factors

Abstract

The factors necessary to maintain organ-specific progenitor cells are poorly understood and yet of extreme clinical importance. Here, we identify the transcription factor SOX9 as the first specific marker and maintenance factor of multipotential progenitors during pancreas organogenesis. In the developing pancreas, SOX9 expression is restricted to a mitotically active, Notch-responsive subset of PDX1 + pluripotent progenitors and is absent from committed endocrine precursors or differentiated cells. Similar to Notch mutations, organ-specific Sox9 inactivation in mice causes severe pancreatic hypoplasia resulting from depletion of the progenitor cell pool. We show that Sox9 maintains pancreatic progenitors by stimulating their proliferation, survival, and persistence in an undifferentiated state. Our finding that SOX9 regulates the Notch-effector HES1 suggests a Notch-dependent mechanism and establishes a possible genetic link between SOX factors and Notch. These findings will be of major significance for the development of in vitro protocols for cell replacement therapies.

Published

2007

29. PAX9 Expression in Potentially Malignant Disorders and Early Stage Squamous Cell Carcinoma of the Oral Cavity

Author

Peter Thomson, Renna Mahsoub, Max Robinson, Timothy Bates, Ralf Kist, and Philip Sloan

Subjects

Gerontology, business.industry, Oral cavity, Pathology and Forensic Medicine, Cancer research, Medicine, Radiology, Nuclear Medicine and imaging, Dentistry (miscellaneous), Surgery, Basal cell, Oral Surgery, Stage (cooking), business, PAX9

Published

2015

30. Reduction of Pax9 gene dosage in an allelic series of mouse mutants causes hypodontia and oligodontia

Author

Donald J. Reid, Paul Cairns, Ralf Kist, Colin G. Miles, Michelle Watson, Xiaomeng Wang, and Heiko Peters

Subjects

Transcription, Genetic, Mutant, Molecular Sequence Data, Gene Dosage, Oligodontia, Biology, Gene dosage, Mice, stomatognathic system, Genetics, medicine, Morphogenesis, Animals, Paired Box Transcription Factors, RNA, Messenger, Allele, Dental Enamel, Molecular Biology, Genetics (clinical), Alleles, Anodontia, Base Sequence, General Medicine, medicine.disease, Null allele, Mice, Mutant Strains, Incisor, stomatognathic diseases, Hypodontia, Mutation, Molar, Third, PAX9 Transcription Factor, Haploinsufficiency, PAX9, Tooth

Abstract

Missing teeth (hypodontia and oligodontia) are a common developmental abnormality in humans and heterozygous mutations of PAX9 have recently been shown to underlie a number of familial, non-syndromic cases. Whereas PAX9 haploinsufficiency has been suggested as the underlying genetic mechanism, it is not known how this affects tooth development. Here we describe a novel, hypomorphic Pax9 mutant allele (Pax9neo) producing decreased levels of Pax9 wild-type mRNA and show that this causes oligodontia in mice. Homozygous Pax9neo mutants (Pax9neo/neo) exhibit hypoplastic or missing lower incisors and third molars, and when combined with the null allele Pax9lacZ, the compound mutants (Pax9neo/lacZ) develop severe forms of oligodontia. The missing molars are arrested at different developmental stages and posterior molars are consistently arrested at an earlier stage, suggesting that a reduction of Pax9 gene dosage affects the dental field as a whole. In addition, hypomorphic Pax9 mutants show defects in enamel formation of the continuously growing incisors, whereas molars exhibit increased attrition and reparative dentin formation. Together, we conclude that changes of Pax9 expression levels have a direct consequence for mammalian dental patterning and that a minimal Pax9 gene dosage is required for normal morphogenesis and differentiation throughout tooth development.

Published

2005

31. Sox9 is required for precursor cell expansion and extracellular matrix organization during mouse heart valve development

Author

Joy Lincoln, Ralf Kist, Gerd Scherer, and Katherine E. Yutzey

Subjects

endocrine system, animal structures, Cellular differentiation, Population, 030204 cardiovascular system & hematology, Biology, Article, Extracellular matrix, Mice, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Precursor cell, FLOX, medicine, Animals, Gene Silencing, Transgenes, Heart valve, education, Molecular Biology, 030304 developmental biology, Heart valves, Extracellular Matrix Proteins, 0303 health sciences, education.field_of_study, Mesenchymal stem cell, High Mobility Group Proteins, Gene Expression Regulation, Developmental, Cell Differentiation, Mesenchymal Stem Cells, SOX9 Transcription Factor, Cell Biology, musculoskeletal system, Immunohistochemistry, Molecular biology, 3. Good health, Cell biology, medicine.anatomical_structure, Cartilage, embryonic structures, Transcription factor, Transcription Factors, Developmental Biology, Extracellular matrix organization, Sox9

Abstract

Heart valve structures derived from mesenchymal cells of the endocardial cushions (ECs) are composed of highly organized cell lineages and extracellular matrix. Sox9 is a transcription factor required for both early and late stages of cartilage formation that is also expressed in the developing valves of the heart. The requirements for Sox9 function during valvulogenesis and adult valve homeostasis in mice were examined by conditional inactivation of Sox9 using Tie2-cre and Col2a1-cre transgenes. Sox9flox/flox;Tie2-cre mice die before E14.5 with hypoplastic ECs, reduced cell proliferation and altered extracellular matrix protein (ECM) deposition. Sox9flox/flox;Col2a1-cre mice die at birth with thickened heart valve leaflets, reduced expression of cartilage-associated proteins and abnormal ECM patterning. Thickened valve leaflets and calcium deposits, characteristic of valve disease, are observed in heterozygous adult Sox9flox/+;Col2a1-cre mice. Therefore, Sox9 is required early in valve development for expansion of the precursor cell population and later is required for normal expression and distribution of valvular ECM proteins. These data indicate that Sox9 is required for early and late stages of valvulogenesis and identify a potential role for Sox9 in valve disease mechanisms.